A heterodimeric complex that promotes the assembly of mammalian 20S proteasomes

被引:0
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作者
Yuko Hirano
Klavs B. Hendil
Hideki Yashiroda
Shun-ichiro Iemura
Ryoichi Nagane
Yusaku Hioki
Tohru Natsume
Keiji Tanaka
Shigeo Murata
机构
[1] Tokyo Metropolitan Institute of Medical Science,Laboratory of Frontier Science, Core Technology and Research Center
[2] University of Copenhagen,Institute of Molecular Biology and Physiology
[3] Biological Information Research Center,National Institute of Advanced Industrial Science and Technology
[4] PRESTO,undefined
[5] Japan Science and Technology Agency,undefined
来源
Nature | 2005年 / 437卷
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摘要
The 26S proteasome is a multisubunit protease responsible for regulated proteolysis in eukaryotic cells1,2. It comprises one catalytic 20S proteasome and two axially positioned 19S regulatory complexes3. The 20S proteasome is composed of 28 subunits arranged in a cylindrical particle as four heteroheptameric rings, α1–7β1–7β1–7α1–7 (refs 4, 5), but the mechanism responsible for the assembly of such a complex structure remains elusive. Here we report two chaperones, designated proteasome assembling chaperone-1 (PAC1) and PAC2, that are involved in the maturation of mammalian 20S proteasomes. PAC1 and PAC2 associate as heterodimers with proteasome precursors and are degraded after formation of the 20S proteasome is completed. Overexpression of PAC1 or PAC2 accelerates the formation of precursor proteasomes, whereas knockdown by short interfering RNA impairs it, resulting in poor maturation of 20S proteasomes. Furthermore, the PAC complex provides a scaffold for α-ring formation and keeps the α-rings competent for the subsequent formation of half-proteasomes. Thus, our results identify a mechanism for the correct assembly of 20S proteasomes.
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页码:1381 / 1385
页数:4
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